Down-modulation of CD8 beta-chain in response to an altered peptide ligand enables developing thymocytes to escape negative selection

Barnden, MJ; Heath, WR; Carbone, FR

Author(s): Barnden, MJ; Heath, WR; Carbone, FR;
Details: Publication Year 1997-02-01,Volume 175,Issue #2,Page 111-119
Journal Title: CELLULAR IMMUNOLOGY
Publication Type: Journal Article
Abstract: Mice expressing a K-b-restricted transgenic T cell receptor (TCR) and a naturally occurring MHC class I variant molecule, K-bm8, were used to study thymic selection, The transgenic TCR was specific for the major peptide determinant from ovalbumin (OVA(257-264)), while K-bm8 has a mutation that alters the position 2 binding pocket of the K-b molecule, abolishing antigenic peptide presentation and positive selection of transgenic T cells, Peptide presentation was restored by identifying a position 2 analog peptide with K-bm8-binding capacity, In combination with K-bm8, the E2 peptide variant was capable of deleting immature double-positive thymocytes in suspension culture. Similarly, addition of exogenous E2 peptide to fetal thymic organ culture resulted in efficient deletion of double-positive thymocytes, However, there remained a population of CD8 single-positive T cells that exhibited impaired responsiveness to the antigenic peptide and lacked expression of the CD8 beta-chain, These results suggest a mechanism whereby developing thymocytes bearing an alpha beta TCR can modify their expression of the CD8 coreceptor to escape thymic deletion and achieve self-tolerance. (C) 1997 Academic Press.
Publisher: ACADEMIC PRESS INC JNL-COMP SUBSCRIPTIONS
Keywords: T-CELL RECEPTOR; MHC CLASS-I; POSITIVE SELECTION; THYMIC SELECTION; RECOGNITION; EXPRESSION; MICE; SPECIFICITY; LYMPHOCYTES; ACTIVATION
Publisher's Version: https://doi.org/10.1006/cimm.1996.1054
Terms of Use/Rights Notice: Refer to copyright notice on published article.

Creation Date: 1997-02-01 12:00:00